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3. Systematic characterization of immunoglobulin loci and deep sequencing of the expressed repertoire in the Atlantic cod (Gadus morhua).

8. Identification of a pharyngeal mucosal lymphoid organ in zebrafish and other teleosts: Tonsils in fish?

9. Potential impact of celiac disease genetic risk factors on T cell receptor signaling in gluten-specific CD4+ T cells

11. Plasma Cells Are the Most Abundant Gluten Peptide MHC-expressing Cells in Inflamed Intestinal Tissues From Patients With Celiac Disease

12. High-throughput sequencing of insect specimens with sub-optimal DNA preservation using a practical, plate-based Illumina-compatible Tn5 transposase library preparation method.

16. Disease-driving [CD4.sup.+] T cell clonotypes persist for decades in celiac disease

18. Innate lymphoid cell characterization in the rat and their correlation to gut commensal microbes

25. Systematic Prioritization of Candidate Genes in Disease Loci Identifies as a Master Regulator of IFNγ Signaling in Celiac Disease

31. Lung CD4+ T cells in patients with lung fibrosis produce pro-fibrotic IL-13 together with IFNγ

37. B cell tolerance and antibody production to the celiac disease autoantigen transglutaminase 2

38. Characterization of T‐cell receptor transgenic mice recognizing immunodominant HLA‐DQ2.5‐restricted gluten epitopes.

40. Cytokine release and gastrointestinal symptoms after gluten challenge in celiac disease

41. Resident memory CD8 T cells persist for years in human small intestine

43. Resident memory CD8 T cells persist for years in human small intestine

46. Systematic Prioritization of Candidate Genes in Disease Loci Identifies TRAFD1 as a Master Regulator of IFNγ Signaling in Celiac Disease.

47. A TCRα framework–centered codon shapes a biased T cell repertoire through direct MHC and CDR3β interactions

49. Sa1396 A Single Intradermal (ID) Injection of Nexvax2®, a Peptide Composition With Dominant Epitopes for Gluten-Reactive CD4+ T Cells, Activates T Cells and Triggers Acute Gastrointestinal Symptoms in HLA-DQ2.5+ People With Celiac Disease (CeD)

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